Enzyme Changes in Zymogen Granules and in Pancreatic Secretion Throughout Long-Term CCK Treatment

Enzyme Changes in Zymogen Granules and in Pancreatic Secretion Throughout Long-Term CCK Treatment

De Dios, I., A. Rodriguez, A. Garcia-Montero, A. Orfao and M. A. Manso. Enzyme changes in zymogen granules and in pancreatic secretion throughout long-term CCK treatment. Peptides 18(1) 101–110, 1997.—Pancreatic enzyme storage and secretion were studied in rats treated twice daily with SC injections...

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Veröffentlicht in:Peptides (New York, N.Y. : 1980) N.Y. : 1980), 1997, Vol.18 (1), p.101-110
Hauptverfasser: De Dios, Isabel, Rodriguez, Ana, Garcia-Montero, Andres, Orfao, Alberto, Manso, Manuel Antonio
Format: Artikel
Sprache:eng
Schlagworte:
Amylases - metabolism
Animals
Antibodies - immunology
Antibodies - metabolism
CCK
Cytoplasmic Granules - enzymology
Cytoplasmic Granules - metabolism
Enzyme Precursors
Enzymes
Flow Cytometry
Immunodiffusion
Male
Organ Size - drug effects
Pancreas - drug effects
Pancreas - enzymology
Pancreas - metabolism
Pancreatic Juice - metabolism
Pancreatic secretion
Phycoerythrin - metabolism
Rat
Rats
Rats, Wistar
Sincalide - pharmacology
Trypsin - metabolism
Trypsinogen - metabolism
Zymogen granules
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Zusammenfassung:De Dios, I., A. Rodriguez, A. Garcia-Montero, A. Orfao and M. A. Manso. Enzyme changes in zymogen granules and in pancreatic secretion throughout long-term CCK treatment. Peptides 18(1) 101–110, 1997.—Pancreatic enzyme storage and secretion were studied in rats treated twice daily with SC injections (5 μg/kg) of CCK-8 for 3, 7, and 15 days. Isolated zymogen granules were analyzed by flow cytometry to determine their FSC (forward scatter), SSC (side scatter), and amylase and trypsinogen contents. DNA content, pancreatic weight, and both basal and stimulated pancreatic secretion under IV CCK infusion (1.25 μg/kg/h) were also studied. Two subsets of zymogen granules were identified by flow cytometry in both control and CCK-treated rats on the basis of FSC and SSC parameters: Z 1 (smaller and less complex) and Z 2. Both subsets displayed a high degree of heterogeneity with respect to their enzyme content per zymogen granule. During the first 7 days of CCK treatment, hyperplasia and hypertrophy developed in the rats together with changes in the zymogen granules, reflected by a significantly decreased FSC, an increased SSC, and an increase in the mean trypsinogen/amylase ratio per granule. A rise in pancreatic enzyme secretion, especially of trypsin, was observed. After 15 days of CCK administration, a simultaneous decrease in amylase content and increase in trypsinogen content per zymogen granule was observed. A desensitization of the pancreas to CCK happened after 15 days of CCK administration, reflected by a reduction of all the pancreatic functions that had been increased at shorter CCK administration periods. Nevertheless, trypsinogen appeared resistant to desensitization because its secretion significantly increased in response to an IV infusion of CCK. CCK treatment displayed a differential packaging of the enzymes in individual zymogen granules; the trypsinogen/amylase ratio was significantly higher in Z 2 zymogen granules than in Z 1 subset throughout the treatment.
ISSN:0196-9781
1873-5169
DOI:10.1016/S0196-9781(96)00249-5